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  • How singing can benefit mothers with postnatal depression – inkl

    How singing can benefit mothers with postnatal depression – inkl

    1. How singing can benefit mothers with postnatal depression  inkl
    2. Healing power of choirs may extend to postnatal depression  The Times
    3. ‘It gave me my voice back’: How group singing is helping new mums with postnatal depression  BBC
    4. The simple…

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  • Pixel 10 Pro Fold explodes after bend test, fails durability check

    Pixel 10 Pro Fold explodes after bend test, fails durability check

    Google’s Pixel 10 Pro Fold became the first smartphone to explode during a JerryRigEverything durability test, marking a shocking moment in YouTuber Zack Nelson’s decade-long history of stress-testing devices.

    Known for pushing phones to…

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  • Nikkei 225, Kospi, Hang Seng Index, Nifty 50

    Nikkei 225, Kospi, Hang Seng Index, Nifty 50

    SHANGHAI, CHINA – AUGUST 14, 2025 – Tourists are visiting the Bund in Shanghai, China on August 14, 2025.

    Cfoto | Future Publishing | Getty Images

    Asia-Pacific markets opened higher Wednesday, breaking ranks with Wall Street’s declines after U.S. and China exchanged blows in a renewed trade feud.

    U.S. President Donald Trump on Tuesday stateside criticized China for not buying soybeans, calling it an “an economically hostile act.” He also threatened “retribution” such as a cooking oil embargo.

    “Volatility remains elevated, and the best explanation is the strained relationship between the U.S. and China,” Veteran investor Louis Navellier wrote in a note published Wednesday.

    Japan’s benchmark Nikkei 225 index rose 0.3%, while the Topix added 0.75%. South Korea’s Kospi jumped 0.8%, while the small-cap Kosdaq added 0.83%.

    Australia’s ASX/S&P 200 was up 0.93%.

    Hong Kong’s Hang Seng Index was set to open higher, with its futures contract trading at 25,763, against the index’s previous close of 25,441.35.

    Investors will be keeping an eye on China’s inflation data for September coming out later in the morning.

    Overnight in the U.S., the S&P 500 closed down 0.2% to 6,644.31 in a wild day that saw the benchmark fall as much as 1.5% and gain 0.4% at its highs.

    The Nasdaq Composite was off by 0.8% to 22,521.70, although at one point it had fallen as much as 2.1%.The Dow Jones Industrial average closed up 0.4%, or 202.88 points, to 46,270.46 after gaining nearly 1% at one point.

    Federal Reserve Chair Jerome Powell on Tuesday suggested the central bank is nearing a point where it will stop reducing the size of its bond holdings, and provided a few hints that more interest rate cuts are in the cards.

    — CNBC’s Liz Napolitano and Fred Imbert contributed to this report.

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  • Gold Trades Near Record on Fed Rate-Cut Sign, US-China Tensions – Bloomberg.com

    1. Gold Trades Near Record on Fed Rate-Cut Sign, US-China Tensions  Bloomberg.com
    2. Gold breaks $4,100 to hit high on trade jitters, rate-cut optimism  Reuters
    3. Gold steadies above $4,100 as Powell strikes neutral-dovish tone  FXStreet
    4. Gold Analysis Today 13/10:The Gold Market is Preparing  DailyForex
    5. ‘All that glitters is fear’ as $5,000 gold is now ‘increasingly inevitable’ – Societe Generale  KITCO

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  • EU Approval Sought for Relacorilant in Platinum-Resistant Ovarian Cancer

    EU Approval Sought for Relacorilant in Platinum-Resistant Ovarian Cancer

    A marketing authorization application (MAA) for the use of relacorilant in patients with platinum-resistant ovarian cancer has been submitted to the European Medicines Agency, according to an announcement from Corcept Therapeutics Incorporated.1

    The submission was supported by findings from the phase 3 ROSELLA study (GOG-3073/ENGOT ov72/APGOT-Ov10/LACOG-0223/ANZGOG-2221/2023; NCT05257408) and phase 2 studies, which showed that when the selective glucocorticoid receptor antagonist was paired with nab-paclitaxel (Abraxane), it improved progression-free survival (PFS) and overall survival (OS) vs nab-paclitaxel alone. Relacorilant was also found to have favorable tolerability, in line with its known toxicity profile.

    “Our MAA submission brings us a step closer to our goal of delivering relacorilant to patients with platinum-resistant ovarian cancer,” Joseph Belanoff, MD, chief executive officer of Corcept Therapeutics, stated in a news release. “Better treatment options are urgently needed. Relacorilant has the potential to redefine how platinum-resistant ovarian cancer is treated.”

    Status of Relacorilant in Platinum-Resistant Ovarian Cancer: Top Takeaways

    • Corcept Therapeutics has submitted a marketing authorization application to the EMA for relacorilant plus nab-paclitaxel in platinum-resistant ovarian cancer, following positive phase 3 ROSELLA and other phase 2 data.
    • In ROSELLA, the combination improved median PFS to 6.54 months vs 5.52 months and OS to 15.97 months vs 11.50 months.
    • Relacorilant showed a manageable safety profile, requires no biomarker testing, and is an oral agent that could be easily integrated into current treatment practice.
    • A new drug application for relacorilant in this patient population is also under FDA review.

    What Was the ROSELLA Study Schema?

    The phase 3 trial enrolled patients (n = 381) with epithelial ovarian, primary peritoneal or fallopian tube cancer who experienced progression within 6 months after their last dose of platinum therapy.2 Patients had an ECOG performance status of 0 or 1, had previously received 1 to 3 lines of therapy, and had prior exposure to bevacizumab (Avastin).

    Participants were randomized 1:1 to receive 150 mg of relacorilant plus 80 mg/m2 of nab-paclitaxel or 100 mg/m2 (n = 188) of nab-paclitaxel alone (n = 193). Treatment continued until disease progression or intolerable toxicity. Stratification factors included prior lines of therapy (1 vs >1) and region (North America vs Europe vs Korea, Australia, and Latin America).

    The dual primary end points of the study were PFS by blinded independent central review and RECIST 1.1 criteria and OS. Secondary end points included investigator-assessed PFS, objective response rate (ORR), duration of response, clinical benefit rate (CBR), response by CA-125 Gynecologic Cancer Intergroup (GCIG) criteria, combined response by GCIG and RECIST criteria, and safety.

    The median patient age was 61 years (range, 26-85) in the relacorilant arm and 62 years (range, 33-86) in the nab-paclitaxel–alone arm. Most patients were White (72.3% vs 69.9%), and slightly more than half were from Europe (56.9% vs 56.5%). About one-third had an ECOG performance status of 1 or 2 (28.2% vs 32.6%), and around 12% had BRCA1/2 mutations (12.2% vs 12.4%). In the experimental arm, 8.0%, 48.9%, and 43.1% of patients received 1, 2, or 3 prior lines of therapy, respectively; in the control arm, these respective rates were 9.3%, 46.1%, and 44.6%. In the experimental arm, 6.9% of patients were primary platinum refractory, 35.6% had received at least 1 prior line of therapy in the platinum-resistant setting, and 4.3% had prior taxane exposure in the platinum-resistant setting; in the control arm, these rates were 6.7%, 42.5%, and 3.6%. Prior therapies received in the combination and monotherapy arms were bevacizumab (100%; 100%), taxanes (99.5%; 99.5%), pegylated liposomal doxorubicin (64.4%; 64.8%), and PARP inhibition (60.6%; 62.2%).

    What Were the Efficacy and Safety Data From ROSELLA?

    The median PFS with relacorilant plus nab-paclitaxel was 6.54 months (95% CI, 5.55-7.43) vs 5.52 months (95% CI, 3.94-5.88) with nab-paclitaxel alone, translating to a 30% reduction in the risk of disease progression or death (HR, 0.70; 95% CI, 0.54-0.91; P = .0076). The hazard ratio for PFS per investigator assessment was 0.71 (P = .0030). The 6-month PFS rates in the respective arms were 52% and 42%; the 12-month PFS rates were 25% and 13%.

    At the time of the interim analysis, which had a data maturity of 50%, the addition of relacorilant to nab-paclitaxel was also found to improve OS over nab-paclitaxel alone, at a median of 15.97 months (95% CI, 13.47-not reached) and 11.50 months (95% CI, 10.02-13.57), respectively (HR, 0.69; 95% CI, 0.52-0.92; nominal P = .0121). The 12-month OS rates in the respective arms were 60% and 49%.

    The relacorilant combination elicited an ORR of 36.9% vs 30.1% with nab-paclitaxel monotherapy, translating to a 6.8% improvement (P = .17). The CBRs in the respective arms were 51.1% and 38.9%, translating to a 12.2% improvement (P = .016).

    In terms of safety, ascites was found to be less common in those given relacorilant vs not, with unadjusted incidence rates of 5% and 11%, respectively, for all-grade ascites; for grade 3 or higher, the rates were 3% and 5%.

    Treatment-emergent adverse effects (TEAEs) occurred in all patients who received the combination (n = 188) vs 99.5% of those who received the monotherapy (n = 190); they were grade 3 or higher for 74.5% and 59.5% of patients, respectively. Serious adverse effects (AEs) were reported in 35.1% of those in the combination arm and 23.7% of those in the monotherapy arm. AEs that resulted in treatment discontinuation for more than 2 patients were intestinal obstruction and paresthesia. No fatal AEs were tied to relacorilant.

    What Is the Significance of Relacorilant in Platinum-Resistant Ovarian Cancer?

    In a past interview with OncLive®, Domenica Lorusso, MD, PhD, of Humanitas Hospital San Pio X in Milan and Humanitas University in Rozzano, Italy, discussed the clinical implications of the ROSELLA data.3 “[Nab-paclitaxel plus relacorilant] can be easily considered a new standard of care for our patients with platinum-resistant and refractory ovarian cancer,” she said. “[What was interesting about] the trial is that the comparator arm was nab-paclitaxel. According to the indirect trial comparison data we have, [this is] as effective as weekly paclitaxel, [which] we consider [to be] the most effective drug in the platinum-resistant setting. What we demonstrate with the ROSELLA trial is that when we add relacorilant to the best drug in the platinum-resistant setting, we further increase PFS.”

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  • Finlay, B. in Encyclopedia of Neuroscience (ed. Squire, L. R.) 337–345 (Academic, 2009).

  • Halley, A. C. & Krubitzer, L. Not all cortical expansions are the same: the coevolution of the neocortex and the dorsal thalamus in mammals. Curr. Opin….

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  • YouTube Rolls Out UI Updates, Threaded Comments, Audio Replies and More

    YouTube Rolls Out UI Updates, Threaded Comments, Audio Replies and More

    YouTube has announced a raft of new updates, including a UI refresh, expanded voice replies, expanded access to courses, an update on fixable violations, and more.

    First off, YouTube’s rolling…

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  • How to Watch ‘Murdaugh: Death in the Family’: Premiere, Schedule, Cast

    How to Watch ‘Murdaugh: Death in the Family’: Premiere, Schedule, Cast

    If you purchase an independently reviewed product or service through a link on our website, The Hollywood Reporter may receive an affiliate commission.

    A new true crime drama is about to hit streaming. Based on what’s commonly referred to…

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  • Intestinal Parasites Symptoms: Do you have intestinal parasites? Gastroenterologist shares common symptoms to be aware of |

    Intestinal Parasites Symptoms: Do you have intestinal parasites? Gastroenterologist shares common symptoms to be aware of |

    Image credits: Getty Images

    Parasites in the intestines. Sounds alarming right? If a gastroenterologist’s words are to go by then it is. According to Dr Joseph Salhab, a gastroenterologist with a following of 1.5M on Instagram, you could be…

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  • Carrie Preston’s Thankful Julia Roberts Was ‘Mean’ Filming Duplicity

    Carrie Preston’s Thankful Julia Roberts Was ‘Mean’ Filming Duplicity

    Carrie Preston said Julia Roberts was “mean” to her on the set of 2009’s Duplicity, but she had a good reason.

    During a recent interview on Jesse Tyler Ferguson’s Dinner’s on Me podcast, the actress recounted her experience…

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